Discovery, Optimization, and Evaluation of Potent and Highly Selective PI3Kγ-PI3Kδ Dual Inhibitors

  • J Med Chem. 2019 May 23;62(10):4936-4948. doi: 10.1021/acs.jmedchem.8b02014.
Hong Jia  1 Guangxiu Dai  1 Weiguo Su  1 Kun Xiao  1 Jianyang Weng  1 Zhulin Zhang  1 Qing Wang  1 Tianhai Yuan  1 Fuying Shi  1 Zheng Zhang  1 Wei Chen  1 Yang Sai  1 Jian Wang  1 Xiong Li  1 Yu Cai  1 Jun Yu  1 Ping Ren  1 Jennifer Venable  2 Tadimeti Rao  2 James P Edwards  3 Scott D Bembenek  2
Affiliations
  • 1. Hutchison MediPharma Limited , Building 4, 720 Cai Lun Road, Zhangjiang Hi-Tech Park , Shanghai 201203 , China.
  • 2. Janssen Pharmaceuticals Research & Development , 3210 Merryfield Row , San Diego , California 92121 , United States.
  • 3. Janssen Pharmaceutical Research & Development , 1400 McKean Road , Spring House , Pennsylvania 19477 , United States.
Abstract

An electronic density model was developed and used to identify a novel pyrrolotriazinone replacement for a quinazolinone, a commonly used moiety to impart selectivity in inhibitors for PI3Kγ and PI3Kδ. Guided by molecular docking, this new specificity piece was then linked to the hinge-binding region of the inhibitor using a novel cyclic moiety. Further structure-activity relationship optimization around the hinge region led to the discovery of candidate 26, a highly potent and selective PI3Kγ-PI3Kδ dual inhibitor with favorable drug metabolism and pharmacokinetic properties in preclinical species.